dbCAN-seq: a database of CAZyme sequence and annotation

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CAZyme Information: MGYG000001453_00484

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Basic Information help

Species

Aneurinibacillus aneurinilyticus

Lineage

Bacteria; Firmicutes; Bacilli; Aneurinibacillales; Aneurinibacillaceae; Aneurinibacillus; Aneurinibacillus aneurinilyticus

CAZyme ID

MGYG000001453_00484

CAZy Family

GT2

CAZyme Description

Linear gramicidin synthase subunit B

CAZyme Property

Protein Length	CGC	Molecular Weight	Isoelectric Point
1722	MGYG000001453_31\|CGC1	195915.09	5.4972

Genome Property

Genome Assembly ID	Genome Size	Genome Type	Country	Continent
MGYG000001453	5302959	Isolate	not provided	not provided

Gene Location

Start: 20562; End: 25730 Strand: -

Full Sequence Download help

MNHSRGYILK KINSISILTA QEREQILFEW NDTEVSYPGD KGLHQLFEEQ VLRTPEHVAA	60
VFGDEQITYD ELNRHSNQLA HYLREIGVQK DTAVGILMER SLDLVVALLG ILKAGGSFLP	120
LDTENPSARI GHILEDAQAT ICITQDHLVD KLSELQWVKP VFFEEQLDFI QSFSQDNLDV	180
SHDPDQLVSI YYTSGSTGNP KGVASTHRGW VNRMDWMQKK HQLTSRETVL QKTTLTFDDA	240
AVEFFWPLMV GARIALMEPG SHRDPRAILD AAIRYDAAVI QFVPSMLRMV LETITPEDKA	300
QLSSLRVVVS SGEALQACLV GEFLEKMPGD LFNSWGATEV SIDSTVHKCS KEDALYGGVV	360
SVGRPINNNQ VYILDSYLQP VPIGVPGDLY LGGVGLAREY INQPKKTNEA FVNNPFVHGT	420
RMYKTGDTGY YTPDGSIMFL GRKDNQIKIR GMRVELGEIE SVLMRCSGIK EAVVDVSGHD	480
DIKRLVAYIV SDDKELNQSK LRSFLSNQLP DYMIPSFYIF LEKLPLNANG KIDRKALPQP	540
DLEQVVSDSD FVAPKTDTEK KLAEIFSRVL GLKRIGIHDN FFALGGHSLL VVKLVSRIQE	600
LFEVRLPLRT IFESPTVEKL SFILDQEQSP RGNITSLMKC DRSQTIPLSY AQRRLWFLNQ	660
LDSENAAYNM PIIMKLNGQL DLEALKQSLR RIIERHEILR TTFKSADGGP VQVIDDTYDI	720
QLNMVDFTSY SKEQRIERAQ DWYRIEARRP FVLSQSPLIR PYLLRLDSQE YALVINVHHI	780
LSDGWSLDIL KHELTCCYEA FVQHREPSLP TLTYQYADYA YSQHQWMKNE EFQRQLAYWK	840
ERLAGDIPLL TLPTDHVPMP TSQEHIRKLP IKLTDDLRQW SEKQGATLFM TMLAVFKILL	900
HRQTGQEDIM VGTPVINRDN QHLEPLIGLF LNTIVLRTQF SRKMSFKEIV HLIRDNFIDD	960
FSHKDVPFEM LVEEVQPNRN LNRSPLFDVF VNYVNFDNNM KPKWNMHNIA MEPLDWLEPV	1020
SKFLLTLYIV ETEEGLVLNF VHQSDAFSAE RVEMWLDQYQ LLLEQMLEQP DQPIHSFSLT	1080
RQYTDGLLPD PTVDLDQPEV QKVYQLISNQ AQQHPNKVSI TQGNKSYTYS QLMEKADQVA	1140
NFLRKRGVQS KQVIAVRGKR SHAFIPIMLG IWKVEGILLL IDSAFPDARQ QSLIQESSAS	1200
WLIDIPLDCH IENYEQNVTM KPLANEAPIN LNLSTDQADL DPAYIFFTSG TTGKPKGVLG	1260
SHQGLSHFLL WQQKEFGIHS QDRAAQLTNL SFDVYLRDTL LILISGGTLC IPEDPYDLHG	1320
ETIISWLKKE KITLIHSVPS ILQSWVMDQQ SQTSLASLRW IFSAGEPLTG SLIEKWRAKF	1380
QQTGTFVNLY GPTETSLAKC FYIVPDSIQQ GILPVGQPIP QTQVLILNEE RSLCGVGEVG	1440
EMVIRTPFRS MGYCNSPDET KRLFSPNHFK NERNDLLYYT GDMGRYRPDG SIEILGRTDD	1500
EIKIRGVKIH PSEISAVIAK HPAVSQCVVV AVKEQSGDHK LFSYIVAKSD TGINDEELRE	1560
YISQELPVSM QPSGFMFLPR LPLTLNGKID RKALPNPVFR ISEVAYVPPS DEIEEKICEV	1620
WASLLNVEKI GIKDNFFSLG GHSLLAVQVV ARIRKTFSID FSVPHLFENP TVAKLAELVR	1680
NSKSSSPLVQ PITKIEKEWD SESIDKLSNE EIEGMIESLM KN	1722

Enzyme Prediction help

No EC number prediction in MGYG000001453_00484.

CDD Domains download full data without filtering help

Cdd ID	Domain	qStart	qEnd	sStart	sEnd	Domain Description
cd17646	A_NRPS_AB3403-like	44	537	1	488	Peptide Synthetase. The adenylation (A) domain of NRPS recognizes a specific amino acid or hydroxy acid and activates it as an (amino) acyl adenylate by hydrolysis of ATP. The activated acyl moiety then forms a thioester bond to the enzyme-bound cofactor phosphopantetheine of a peptidyl carrier protein domain. NRPSs are large multifunctional enzymes which synthesize many therapeutically useful peptides in bacteria and fungi via a template-directed, nucleic acid independent nonribosomal mechanism. These natural products include antibiotics, immunosuppressants, plant and animal toxins, and enzyme inhibitors. NRPS has a distinct modular structure in which each module is responsible for the recognition, activation, and in some cases, modification of a single amino acid residue of the final peptide product. The modules can be subdivided into domains that catalyze specific biochemical reactions.
cd19531	LCL_NRPS-like	645	1070	1	427	LCL-type Condensation (C) domain of non-ribosomal peptide synthetases(NRPSs) and similar domains including the C-domain of SgcC5, a free-standing NRPS with both ester- and amide- bond forming activity. LCL-type Condensation (C) domains catalyze peptide bond formation between two L-amino acids, ((L)C(L)). C-domains of NRPSs catalyze peptide bond formation within (usually) large multi-modular enzymatic complexes. NRPS can use a large variety of acyl monomers (approximately 500 different possible monomer substrates as opposed to the 20 standard amino acids in ribosomal protein synthesis) to construct bioactive secondary metabolites of 2 to 18 units long (with various activities such as antibiotic, antifungal, antitumor and immunosuppression). In addition to the LCL-type, there are various subtypes of C-domains such as the DCL-type which links an L-amino acid to the D-amino acid at the end of a growing peptide, starter C-domains which acylate the first amino acid with a beta-hydroxy carboxylic acid, and heterocyclization (Cyc) domains which catalyze both peptide bond formation and cyclization of Cys, Ser, or Thr residues. Typically, an NRPS module consists of an adenylation domain, a peptidyl carrier protein (PCP) domain (also known as thiolation (T) domain) and a C-domain. NRPS modules may also include specialized domains such as the terminal-module thioesterase (Te) domain that releases the product via hydrolysis or macrocyclization and any of various C-domain family members such as the epimerization (E) domain, the ester-bond forming C-domain, dual E/C (epimerization and condensation) domains, and the X-domain. Streptomyces globisporus SgcC5 is a free-standing NRPS condensation enzyme (rather than a modular NRPS), which catalyzes the condensation between the SgcC2-tethered (S)-3-chloro-5-hydroxy-beta-tyrosine and (R)-1phenyl-1,2-ethanediol, forming an ester bond, during the synthesis of the chromoprotein enediyne antitumor antibiotic C-1027. It has some acceptor substrate promiscuity as it has been shown to also catalyze the formation of an amide bond between SgcC2-tethered (S)-3-chloro-5-hydroxy-beta-tyrosine and a mimic of the enediyne core acceptor substrate having an amine at its C-2 position. C-domains typically have a conserved HHxxxD motif at the active site; mutations in this motif can abolish or diminish condensation activity. An HHxx[SAG]DGxSx(6)[ED] motif is characteristic of LCL-type C-domains.
PRK12467	PRK12467	10	911	1543	2443	peptide synthase; Provisional
PRK12467	PRK12467	11	1693	483	2178	peptide synthase; Provisional
cd05930	A_NRPS	55	537	1	444	The adenylation domain of nonribosomal peptide synthetases (NRPS). The adenylation (A) domain of NRPS recognizes a specific amino acid or hydroxy acid and activates it as an (amino) acyl adenylate by hydrolysis of ATP. The activated acyl moiety then forms a thioester bond to the enzyme-bound cofactor phosphopantetheine of a peptidyl carrier protein domain. NRPSs are large multifunctional enzymes which synthesize many therapeutically useful peptides in bacteria and fungi via a template-directed, nucleic acid independent nonribosomal mechanism. These natural products include antibiotics, immunosuppressants, plant and animal toxins, and enzyme inhibitors. NRPS has a distinct modular structure in which each module is responsible for the recognition, activation, and in some cases, modification of a single amino acid residue of the final peptide product. The modules can be subdivided into domains that catalyze specific biochemical reactions.

CAZyme Hits help

Hit ID	E-Value	Query Start	Query End	Hit Start	Hit End
QND46664.1	9.77e-290	12	1683	980	2666
BAY90071.1	3.95e-185	522	1687	2100	3291
BAY30132.1	3.19e-184	522	1687	2111	3302
BAZ00088.1	9.09e-182	522	1687	2109	3300
BAZ75991.1	9.09e-182	522	1687	2109	3300

PDB Hits download full data without filtering help

Hit ID	E-Value	Query Start	Query End	Hit Start	Hit End	Description
6MFZ_A	1.13e-254	38	1683	202	1801	Crystalstructure of dimodular LgrA in a condensation state [Brevibacillus parabrevis],6MFZ_B Crystal structure of dimodular LgrA in a condensation state [Brevibacillus parabrevis]
6MFY_A	1.65e-234	38	1597	202	1715	Crystalstructure of a 5-domain construct of LgrA in the substrate donation state [Brevibacillus parabrevis],6MG0_A Crystal structure of a 5-domain construct of LgrA in the thiolation state [Brevibacillus parabrevis],6MG0_B Crystal structure of a 5-domain construct of LgrA in the thiolation state [Brevibacillus parabrevis]
5U89_A	7.98e-199	21	1074	5	1056	Crystalstructure of a cross-module fragment from the dimodular NRPS DhbF [Geobacillus sp. Y4.1MC1]
6MFW_A	6.87e-157	38	1079	202	1200	Crystalstructure of a 4-domain construct of LgrA in the substrate donation state [Brevibacillus parabrevis]
6MFX_A	3.46e-156	38	1079	202	1200	Crystalstructure of a 4-domain construct of a mutant of LgrA in the substrate donation state [Brevibacillus parabrevis]

Swiss-Prot Hits download full data without filtering help

Hit ID	E-Value	Query Start	Query End	Hit Start	Hit End	Description
Q70LM4	0.0	10	1679	432	2093	Linear gramicidin synthase subunit D OS=Brevibacillus parabrevis OX=54914 GN=lgrD PE=1 SV=1
Q70LM6	0.0	10	1682	3007	4674	Linear gramicidin synthase subunit B OS=Brevibacillus parabrevis OX=54914 GN=lgrB PE=1 SV=1
Q70LM5	0.0	10	1682	5611	7273	Linear gramicidin synthase subunit C OS=Brevibacillus parabrevis OX=54914 GN=lgrC PE=3 SV=1
P0C064	6.92e-317	11	1704	2512	4184	Gramicidin S synthase 2 OS=Brevibacillus brevis OX=1393 GN=grsB PE=1 SV=2
O30409	5.29e-315	15	1682	1474	3114	Tyrocidine synthase 3 OS=Brevibacillus parabrevis OX=54914 GN=tycC PE=1 SV=1

SignalP and Lipop Annotations help

This protein is predicted as OTHER

Other	SP_Sec_SPI	LIPO_Sec_SPII	TAT_Tat_SPI	TATLIP_Sec_SPII	PILIN_Sec_SPIII
1.000068	0.000000	0.000000	0.000000	0.000000	0.000000

TMHMM Annotations help

There is no transmembrane helices in MGYG000001453_00484.